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草稿:貝賽特氏症

维基百科,自由的百科全书
貝賽特氏症
异名
  • 貝賽特氏病(Behçet disease)
  • 貝賽特氏症(Behçet's syndrome)
  • 絲路病(Silk Road disease)
前房葡萄膜炎為貝賽特氏症的典型特徵,圖中可以看到前房蓄膿英语hypopyon
读音
  • /bɛˈɛt/, 土耳其語:[behˈtʃet]
症状口腔潰瘍、生殖器潰瘍、葡萄膜炎、关节炎[1]慢性疲勞
併發症視覺障礙关节炎血栓動脈瘤[2]
起病年龄20至40歲[1][2]
病程長期[1]
病因不明[1]
診斷方法症狀學診斷[1]
鑑別診斷反应性关节炎史蒂芬斯-強森症候群急性發熱性嗜中性皮病[2]
藥物皮質類固醇免疫抑制劑[1]
预后有時會緩解[2]
患病率亞裔常見,尤見於絲路地帶,歐美罕見[2]
分类和外部资源
醫學專科風濕病學免疫学
[编辑此条目的维基数据]

貝西特氏症(Behçet's disease,BD)是一種會影響身體多個部位的發炎性及病[2]。最常見的症狀包括口腔及其他部位黏膜出現疼痛性潰瘍、眼部炎症,以及關節炎[1][2]。潰瘍可能持續數日,甚至一週以上。較少見的情況下,可能會出現腦部或脊髓的炎症、血栓動脈瘤視覺障礙[1][2]。這些症狀通常呈現反覆發作的情形[1]

目前病因不明[1],可能與基因疾患有關[2]。貝西特氏症並非傳染病[1]。診斷需根據一年內至少三次口腔潰瘍發作,以及下列條件中至少兩項:生殖器潰瘍、眼部發炎、皮膚病變、皮膚針刺試驗英语Pathergy test呈陽性反應[1]

目前尚無治癒性療法。治療方式可能包括免疫抑制劑(如皮質類固醇與抗腫瘤壞死因子藥物)及生活方式調整[1]利多卡因漱口水可幫助緩解疼痛[2]秋水仙素可降低發作頻率[2]

此病在中東與亞洲則較常見,在美國與歐洲較為少見。例如在土耳其,每千人中約有兩人罹患此病[2]。好發年齡通常為二十至四十歲之間[1][2]。該病最早於1937年由土耳其皮膚科醫師胡魯西·貝西特英语Hulusi Behçet所描述。[3]

Signs and symptoms

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Skin and mucosa

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Nearly all people with Behçet's disease present with some form of painful ulcerations inside the mouth.[4] They are a form of aphthous ulcers or non-scarring oral lesions.[4] The oral lesions are similar to those found in inflammatory bowel disease and can be relapsing.[4] Painful genital ulcerations usually develop around the anus, vulva, or scrotum and cause scarring in 75 percent of the patients.[4] Additionally, patients may present with erythema nodosum, cutaneous pustular vasculitis, and lesions similar to pyoderma gangrenosum.[4]

Eyes

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Left eye blood vessels
Funduscopic photo left eye centered on the optic disc英语optic disc

Inflammatory eye disease can develop early in the disease course and lead to permanent vision loss in 20 percent of cases. Ocular involvement can be in the form of posterior uveitis, anterior uveitis, or retinal vasculitis英语retinal vasculitis. Anterior uveitis presents with painful eyes, conjuctival redness, hypopyon英语hypopyon, and decreased visual acuity, while posterior uveitis presents with painless decreased visual acuity and visual field floaters. A rare form of ocular (eye) involvement in this syndrome is retinal vasculitis which presents with painless decrease of vision with the possibility of floaters or visual field defects.[4]

Optic nerve involvement in Behçet's disease is rare, typically presenting as progressive optic atrophy英语optic atrophy and visual loss. However, cases of acute optic neuropathy (specifically anterior ischemic optic neuropathy英语anterior ischemic optic neuropathy) have also been reported to occur.[5] Optic nerve atrophy has been identified as the most common cause of visual impairment. Behçet's disease may result in primary or secondary optic nerve involvement. Papilledema as a result of dural sinus thrombosis[6] and atrophy resulting from retinal disease, have been characterized as secondary causes of optic nerve atrophy in Behçet's disease.[7][8]

Signs and symptoms of acute optic neuropathy英语optic neuropathy include painless loss of vision which may affect either one or both eyes, reduced visual acuity, reduced color vision, relative afferent pupillary defect英语relative afferent pupillary defect, central scotoma英语scotoma, swollen optic disc, macular edema, or retrobulbar pain. When these symptoms occur with concurrent mucocutaneous ulcerations, they raise suspicion of acute optic neuropathy in Behçet's Disease. Progressive optic atrophy may result in decreased visual acuity or color vision. Intracranial hypertension with papilledema may be present.[9]

Episcleritis英语Episcleritis may occur, which causes eye redness and mild pain, without a significant impact on vision.[10]

Bowels

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Gastrointestinal (GI) manifestations include abdominal pain, nausea, and diarrhea with or without blood, and they often involve the terminal ileum and ileocecal valve.[4] Some patients with BD experience abdominal tenderness, bloating, and general abdominal discomfort. When mild this can resemble irritable bowel syndrome; more severe cases bear similarities to inflammatory bowel diseases such as ulcerative colitis or Crohn's. Behçet's disease causes ulcers in the terminal ileum and ileocecal valve. The ulcers may be aphthous or have a classic punched out appearance with undermining. Linear and fissuring ulcers up to 5 cm may be present. Biopsies show vasculitis (phlebitis or venulitis) with a neutrophilic inflammatory infiltrate. Involvement of the oesophagus, stomach and large intestine is rare.[來源請求]

Lungs

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Lung involvement is typically in the form of hemoptysis, pleuritis, cough, or fever, and in severe cases can be life-threatening if the outlet pulmonary artery develops an aneurysm which ruptures causing severe vascular collapse and death from bleeding in the lungs.[4] Pulmonary artery thrombosis may occur.

Joints

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Arthritis is seen in up to half of people, and is usually a non-erosive poly or oligoarthritis primarily of the large joints of the lower extremities.[4]

Kidneys

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Behçet's disease can rarely result in renal involvement. This can manifest in the following:

Small vessel vascular disease results in renal vasculitis, whereas large vessel involvement causes aneurysms (bulging) and thrombosis (blockages). Serious kidney problems are more common in men typically with a history of large vessel involvement in other parts of the body. Bladder and urethral involvement is rare in Behçet's disease.

Brain

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主条目:Neuro-Behçet's disease

Central nervous system (CNS) involvement most often occurs as a chronic meningoencephalitis. Lesions tend to occur in the brainstem, the basal ganglia and deep hemispheric white matter and may resemble those of multiple sclerosis (MS). Brainstem atrophy is seen in chronic cases.[來源請求]

Neurological involvements range from aseptic meningitis英语aseptic meningitis to vascular thrombosis such as dural sinus thrombosis and organic brain syndrome英语organic brain syndrome manifesting with confusion, seizures, and memory loss. Sudden hearing loss (sensorineural) is often associated with it.[4] They often appear late in the progression of the disease but are associated with a poor prognosis.[來源請求]

Heart

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Chronic aortic regurgitation due to aortic root disease may also be seen.[11] Although infrequent, myocardial infarction (heart attack) with angiographically identified acute coronary artery thrombosis has been reported, including one case with a pathologically demonstrable lesion due to arteritis found at autopsy.[12]

Blood vessels

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Blood vessel problems are observed in 7–29% of people with arterial lesions representing 15% of vascular lesions. Arterial lesions pose a greater risk. Most common arterial lesions are occlusions or stenosis and aneurysms or pseudoaneurysms.[13] [來源請求]

Cause

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The cause is not well-defined, but it is primarily characterized by auto-inflammation of the blood vessels. Although sometimes erroneously referred to as a diagnosis of exclusion, the diagnosis can sometimes be reached by pathologic examination of the affected areas.[14]

The primary mechanism of the damage is autoimmune, which by definition is an overactive immune system that targets the patient's own body. The involvement of a subset of T cells (Th17英语Th17) seems to be important.[15] The primary cause is not well known. In fact, no one knows yet why the immune system starts to behave this way in Behçet's disease. There does however seem to be a genetic component involved, as first degree relatives of the affected patients are often affected in more than the expected proportion for the general population.[來源請求]

Research suggests that previous infections may provoke the autoimmune responses present in Behçet's disease. Heat shock proteins (HSPs) are present in some bacteria and serve as a "danger signal" to the immune system. However, some HSPs share a similarity in bacteria and humans.[16] The anti-HSP60英语HSP60 and anti-HSP65 antibodies that target HSPs produced by Streptococci (including S. sanguinis and S. pyogenes) and Mycobacterium tuberculosis can also target human HSPs, leading to immune responses linked to uveitis and various symptoms shown in parenchymal neuro-Behçet's disease.[17]

An association with the GIMAP ("GTPase英语GTPase of the immunity-associated protein") family of genes on the long arm of chromosome 7 (7q36.1) has been reported.[18] Gene locations of single-nucleotide polymorphisms associated with Behçet's disease included GIMAP1, GIMAP2 and GIMAP4英语GIMAP4.[18]

Pathophysiology

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HLA-B51英语HLA-B51 is strongly associated with Behçet's disease[19]

Behçet's disease is considered more prevalent in the areas surrounding the old silk trading routes in the Middle East and in Central Asia. Thus, it is sometimes known as Silk Road disease. However, this disease is not restricted to people from these regions. A large number of serological studies show a linkage between the disease and HLA-B51英语HLA-B51.[20] HLA-B51 is more frequently found from the Middle East to South Eastern Siberia, but the incidence of B51 in some studies was 3 fold higher than the normal population. However, B51 tends not to be found in disease when a certain SUMO4英语SUMO4 gene variant is involved,[21] and symptoms appear to be milder when HLA-B27 is present.[22] At the current time, a similar infectious origin has not yet been confirmed that leads to Behçet's disease, but certain strains of S. sanguinis has been found to have a homologous antigenicity.[23]

Vasculitis resulting in occlusion of the vessels supplying the optic nerve may be the cause of acute optic neuropathy and progressive optic atrophy in Behçet's disease. Histological evaluation in a reported case of acute optic neuropathy demonstrated substitution of the axonal portion of the optic nerve with fibrous astrocytes without retinal changes.[8] CNS involvement in Behçet's disease may lead to intracranial hypertension most commonly due to dural venous sinus thrombosis[6] and subsequent secondary optic atrophy.

Diagnosis

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There is no specific pathological testing or technique available for the diagnosis of the disease, although the International Study Group criteria for the disease are highly sensitive and specific, involving clinical criteria and a pathergy英语pathergy test.[4][24] Behçet's disease has a high degree of resemblance to diseases that cause mucocutaneous lesions such as Herpes simplex labialis, and therefore clinical suspicion should be maintained until all the common causes of oral lesions are ruled out from the differential diagnosis.[來源請求]

Visual acuity, or color vision loss with concurrent mucocutaneous lesions or systemic Behçet's disease symptoms should raise suspicion of optic nerve involvement in Behçet's disease and prompt a work-up for Behçet's disease if not previously diagnosed in addition to an ocular work-up. Diagnosis of Behçet's disease is based on clinical findings including oral and genital ulcers, skin lesions such as erythema nodosum, acne, or folliculitis, ocular inflammatory findings and a pathergy reaction. Inflammatory markers such ESR, and CRP may be elevated. A complete ophthalmic examination may include a slit lamp examination, optical coherence tomography to detect nerve loss, visual field examinations, fundoscopic examination to assess optic disc atrophy and retinal disease, fundoscopic angiography, and visual evoked potentials, which may demonstrate increased latency. Optic nerve enhancement may be identified on Magnetic Resonance Imaging (MRI) in some patients with acute optic neuropathy. However, a normal study does not rule out optic neuropathy. Cerebrospinal fluid (CSF) analysis may demonstrate elevated protein level with or without pleocytosis. Imaging including angiography may be indicated to identify dural venous sinus thrombosis as a cause of intracranial hypertension and optic atrophy.[來源請求]

Diagnostic guidelines

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Magnetic resonance venogram demonstrating occlusion of the left sigmoid and transverse sinuses

According to the International Study Group guidelines, for a patient to be diagnosed with Behçet's disease,[24] the patient must have oral (aphthous) ulcers (any shape, size, or number at least three times in any twelve-month period) along with two of the following four hallmark symptoms:[來源請求]

Despite the inclusive criteria set forth by the International Study Group, there are cases where not all the criteria can be met and therefore a diagnosis cannot readily be made. There is, however, a set of clinical findings that a physician can rely upon in making a tentative diagnosis of the disease; essentially, Behçet's disease does not always follow the International Study Group guidelines and so a high degree of suspicion for a patient who presents having any number of the following findings is necessary:[來源請求]

Treatment

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Current treatment is aimed at easing the symptoms, reducing inflammation, and controlling the immune system. The quality of the evidence for treating the oral ulcers associated with Behçet's disease, however, is poor.[25]

High-dose corticosteroid therapy is often used for severe disease manifestations.[26] Anti-TNF英语TNF inhibitor therapy such as infliximab has shown promise in treating the uveitis associated with the disease.[27][28] Infliximab as well as other anti-TNF therapies including etanercept and adalimumab may be useful in treating mucocutaneous英语mucocutaneous disease according to several case reports and prospective studies, as well as one randomized trial for etanercept.[29][30][31] Apremilast英语Apremilast may also be used to treat oral ulcers associated with Behçet's disease.[32]

Interferon alpha-2a may also be an effective alternative treatment, particularly for the genital and oral ulcers[33] as well as ocular lesions.[34] Azathioprine, when used in combination with interferon alpha-2b also shows promise,[35] and colchicine can be useful for treating some genital ulcers, erythema nodosum, and arthritis.[36] Benzathine-penicillin may also reduce new arthritic attacks.[37]

Thalidomide has also been used due to its immune-modifying effect.[38] Dapsone and rebamipide英语rebamipide have been shown, in small studies, to have beneficial results for mucocutaneous lesions.[39][40]

Given its rarity, the optimal treatment for acute optic neuropathy in Behçet's disease has not been established. Early identification and treatment are essential. Response to ciclosporin, periocular triamcinolone, and IV methylprednisolone followed by oral prednisone has been reported although relapses leading to irreversible visual loss may occur even with treatment.[41] Immunosuppressants such as interferon-alpha and tumour necrosis factor antagonists may improve though not completely reverse symptoms of ocular Behçet's disease, which may progress over time despite treatment. When symptoms are limited to the anterior chamber of the eye prognosis is improved. Posterior involvement, particularly optic nerve involvement, is a poor prognostic indicator. Secondary optic nerve atrophy is frequently irreversible. Lumbar puncture or surgical treatment may be required to prevent optic atrophy in cases of intracranial hypertension refractory to treatment with immunomodulators and steroids.[來源請求]

Intravenous immunoglobulin therapy (IVIg) could be a treatment for severe[42] or complicated cases.[43][44]

A recent 2024 reports that infliximab improved the likelihood of achieving a complete response at 22 weeks for patients with severe Behçet’s syndrome compared to cyclophosphamide, according to head-to-head trial data.[45] Mild to moderate adverse events, primarily infections, were reported in 29.6% of patients on infliximab and 64% on cyclophosphamide. Serious adverse events occurred in 15% and 12% of patients, respectively. [46]

Surgery

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Surgical treatment of arterial manifestations of BD bears many pitfalls since the obliterative endarteritis of vasa vasorum causes thickening of the medial layer and splitting of elastin fibers. Therefore, anastomotic pseudoaneurysms are likely to form, as well as pseudoaneurysms at the site of the puncture in case of angiography or endovascular treatment; furthermore, early graft occlusion may occur.[來源請求]

For these reasons, invasive treatment should not be performed in the acute and active phases of the disease when inflammation is at its peak. The evaluation of disease's activity is usually based on relapsing symptoms, ESR (erythrocyte sedimentation rate), and serum levels of CRP (C-reactive protein).[來源請求]

Endovascular treatment can be an effective and safe alternative to open surgery, with less postoperative complications, faster recovery time, and reduced need for intensive care, while offering patency rates and procedural success rates comparable with those of surgery. This notwithstanding, long-term results of endovascular treatment in BD are still to be determined.[來源請求]

Epidemiology

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The syndrome is rare in the United States, Africa and South America, but is common in Asia, suggesting a possible cause endemic to those areas.[47] A theory suggested that past exposure to lethal infectious agents might have fixed the genetic susceptibility factors to Behçet's disease in those area.[48] An estimated 15,000 to 20,000 Americans have been diagnosed with this disease. In the UK, it is estimated to have about 1 case for every 100,000 people.[49]

In an epidemiologic study, 56 percent of patients with Behçet's disease developed ocular involvement at a mean age of 30.[50] Ocular involvement was the first manifestation of Behçet's disease in 8.6 percent of patients.[50] Ocular Behçet's disease with involvement of the optic nerve is rarely reported. Among patients with ocular Behçet's disease funduscopic findings of optic atrophy, and optic disc paleness have been identified with a frequency of 17.9 percent and 7.4 percent, respectively. Other fundoscopic findings include vascular sheathing (23.7%),[7] retinal hemorrhage (9%),[7] macular edema (11.3%),[7] branch retinal vein occlusion (5.8%),[7] and retinal edema (6.6%).[7] However, optic atrophy was the most significant cause of visual impairment identified in 54 percent of patients with ocular Behçet's disease and permanent visual impairment.[7]

Pregnancy

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With Behçet's disease as a pre-existing disease in pregnancy英语pre-existing disease in pregnancy or acquired, the pregnancy does not have an adverse effect on the course of Behçet's disease and may possibly ameliorate its course.[51][52] Still, there is a substantial variability in clinical course between patients and even for different pregnancies in the same patient.[51] Also, the other way around, Behçet's disease confers an increased risk of pregnancy complications, miscarriage and Cesarean section.[52]

Behçet's can cause infertility, either as a result of the condition itself or of a side effect of concomitant medication such as colchicine, which is known to lower sperm count.[53]

History

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The first modern formal description of the symptoms was made by H. Planner and F. Remenovsky and published in 1922 in the Archiv für Dermatologie und Syphilis英语Archiv für Dermatologie und Syphilis.[54] Behçet's disease is named after Hulusi Behçet英语Hulusi Behçet (1889–1948), the Turkish dermatologist and scientist who first recognized the three main symptoms of the syndrome in one of his patients in 1924 and reported his research on the disease in Journal of Skin and Venereal Diseases in 1936.[54][55] The name (Morbus Behçet) was formally adopted at the International Congress of Dermatology in Geneva in September 1947. Symptoms of this disease may have been described by Hippocrates in the 5th century BC, in his Epidemion (book 3, case 7).[56]

Some sources use the term "Adamantiades's syndrome" or "Adamantiades–Behçet syndrome", for the work done by Benediktos Adamantiades英语Benediktos Adamantiades.[57] However, the current World Health Organization/ICD-10 standard is "Behçet's disease". In 1991, Saudi Arabian medical researchers described neuro-Behçet's disease英语neuro-Behçet's disease,[58] a neurological involvement in Behçet's disease, considered one of the most devastating manifestations of the disease.[59] The mechanism can be immune-mediated or thrombotic.[60] The term dates back to at least 1990.[61]

References

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  1. ^ 1.00 1.01 1.02 1.03 1.04 1.05 1.06 1.07 1.08 1.09 1.10 1.11 1.12 1.13 Fleming, Ray. Fast Facts About Behçet's Disease. www.niams.nih.gov. November 2014 [29 May 2017]. (原始内容存档于13 May 2017) (英语). 
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  4. ^ 4.00 4.01 4.02 4.03 4.04 4.05 4.06 4.07 4.08 4.09 4.10 4.11 Bolster MB. MKSAP 15 Medical Knowledge Self-assessment Program: Rheumatology. Philadelphia: American College of Physicians. 2009. ISBN 978-1-934465-30-1. 
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  13. ^ ElGuindy MS, ElGuindy AM. Aneurysmal coronary artery disease: An overview. Global Cardiology Science and Practice (Glob Cardiol Sci Pract.). October 2017, 2017 (3): e201726. PMC 5856968可免费查阅. PMID 29564347. doi:10.21542/gcsp.2017.26可免费查阅. 
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  19. ^ Ohno S, Ohguchi M, Hirose S, Matsuda H, Wakisaka A, Aizawa M. Close association of HLA-Bw51 with Behçet's disease. Arch. Ophthalmol. September 1982, 100 (9): 1455–8. PMID 6956266. doi:10.1001/archopht.1982.01030040433013. 
  20. ^ Durrani K, Papaliodis GN. The genetics of Adamantiades–Behcet's disease. Semin Ophthalmol. 2008, 23 (1): 73–9. PMID 18214795. S2CID 11695492. doi:10.1080/08820530701745264. 
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  23. ^ Yanagihori H, Oyama N, Nakamura K, Mizuki N, Oguma K, Kaneko F. Role of IL-12B promoter polymorphism in Adamantiades-Behcet's disease susceptibility: An involvement of Th1 immunoreactivity against Streptococcus Sanguinis antigen. J. Invest. Dermatol. July 2006, 126 (7): 1534–40. PMID 16514412. doi:10.1038/sj.jid.5700203可免费查阅. 
  24. ^ 24.0 24.1 International Study Group for Behçet's Disease. Criteria for diagnosis of Behçet's disease. Lancet. May 1990, 335 (8697): 1078–80. PMID 1970380. S2CID 53261546. doi:10.1016/0140-6736(90)92643-V. 
  25. ^ Taylor J, Glenny AM, Walsh T, Brocklehurst P, Riley P, Gorodkin R, Pemberton MN. Taylor J , 编. Interventions for the management of oral ulcers in Behçet's disease. The Cochrane Database of Systematic Reviews. 25 September 2014, 9 (9): CD011018. PMC 6872426可免费查阅. PMID 25254615. doi:10.1002/14651858.CD011018.pub2. 
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Further reading

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外部連結

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维基共享资源上的相关多媒体资源:貝賽特氏症
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